MicroRNA signature and integrative omics analyses define prognostic clusters and key pathways driving prognosis in patients with neuroendocrine neoplasms

Citation

Soldevilla, B., Lens-Pardo, A., Espinosa-Olarte, P., Carretero-Puche, C., Molina-Pinelo, S., Robles, C., Benavent, M., Gomez-Izquierdo, L., Fierro-Fernández, M., Morales-Burgo, P., Jimenez-Fonseca, P., Anton-Pascual, B., Rodriguez-Gil, Y., Teijo-Quintans, A., La Salvia, A., Rubio-Cuesta, B., Riesco-Martínez, M.C. and Garcia-Carbonero, R. (2023), MicroRNA signature and integrative omics analyses define prognostic clusters and key pathways driving prognosis in patients with neuroendocrine neoplasms. Mol Oncol, 17: 582-597. https://doi.org/10.1002/1878-0261.13393

Abstract

Neuroendocrine neoplasms (NENs) are mutationally quiet (low number of mutations/Mb), and epigenetic mechanisms drive their development and progression. We aimed at comprehensively characterising the microRNA (miRNA) profile of NENs, and exploring downstream targets and their epigenetic modulation. In total, 84 cancer-related miRNAs were analysed in 85 NEN samples from lung and gastroenteropancreatic (GEP) origin, and their prognostic value was evaluated by univariate and multivariate models. Transcriptomics (N = 63) and methylomics (N = 30) were performed to predict miRNA target genes, signalling pathways and regulatory CpG sites. Findings were validated in The Cancer Genome Atlas cohorts and in NEN cell lines. We identified a signature of eight miRNAs that stratified patients in three prognostic groups (5-year survival of 80%, 66% and 36%). Expression of the eight-miRNA gene signature correlated with 71 target genes involved in PI3K–Akt and TNFα–NF-kB signalling. Of these, 28 were associated with survival and validated in silico and in vitro. Finally, we identified five CpG sites involved in the epigenetic regulation of these eight miRNAs. In brief, we identified an 8-miRNA signature able to predict survival of patients with GEP and lung NENs, and identified genes and regulatory mechanisms driving prognosis in NEN patients.

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Acknowledgements: BS is funded by the AECC (POSTDO46SOLD, Spain). AL-P is funded by the Instituto de Salud Carlos III (PFIS; FI20/00131). ALS is funded by the Instituto de Salud Carlos III (Contrato Rio Hortega). CC-P was partially funded by CAM (PEJD-2016-PRE/BMD-2666). BR-C was partially funded by CAM (PEJD-2017-PRE/BMD-4981). MCR-M is funded by the AECC (CLSEN19003RIES). SM-P was supported by the Consejería de Salud y Familias of the Junta de Andalucía through the ‘Nicolás Monardes’ program (RC-0004-2020).

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